Pathology of Genetically Engineered and Other Mutant Mice. Группа авторов
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Название: Pathology of Genetically Engineered and Other Mutant Mice
Автор: Группа авторов
Издательство: John Wiley & Sons Limited
Жанр: Биология
isbn: 9781119624592
isbn:
Understanding Diseases Found in Mutant Animals
Naturally occurring and induced changes in genes often result in a specific phenotype at the clinical and histopathological levels. The cause of this phenomenon is that genes have specific functions that play a role in the normal homeostasis of cells, tissues, and organs. A genetically engineered mouse () line represents a tool to investigate the effects resulting from the partial or complete loss of gene function or the gain of normal or abnormal functions. The genes are often found to function in specific cellular organelles and biochemical/molecular pathways important for normal biological functions (Figure 1.1) [10]. Cells involved in common gene functions can be single cell types in single tissues, multiple cells types in a single tissue, or multiple cells types in multiple tissues. Gene expression can also be induced in specific cells and tissues by normal and abnormal body functions, or by exposure to external factors such as drugs, infectious agents, environmental modifications, and ingested foods.
Mutant mice often exhibit histopathological changes (lesions) in tissues and organs that are associated with gene function, but the ultimate clinical phenotype can be influenced by various factors. Much of the histopathology found in mutant mice is in the usual spectrum of degenerative, inflammatory, proliferative, and neoplastic changes also found in nonmutant mice. Nouvelle lesions do occur commonly in some lines of mutant mice. These include unique developmental changes, cellular morphological changes, patterns of lesions, types of proliferative lesions, and often strain specific cancer types. These may be due to specific naturally occurring mutations (polymorphisms) in genes that can serve as genetic based models for disease. Spontaneous mutants made up the bulk of mouse models until the advent first of radiation and then chemical mutagenesis programs. The spectrum of spontaneous lesions is noted in each organ‐specific chapter. Often the lesions are identical or very similar to those associated human genetic disorders, but they also may vary from human lesions. The genetic background of the mice often plays a role in spontaneous as well as induced disease phenotypes.
Figure 1.1 Classes of proteins associated with human genetic diseases.
Source: Nussbaum (2007). Reprinted with permission of Elsevier
Mouse Pathology – Nomenclature
The pathology of mice in research was first led by Thelma Dunn and Harold Stewart at the National Cancer Institute (NCI) at the NIH [11–13]. Both were MD pathologists who applied general rules of human pathology diagnosis to mice when possible. Although mouse pathology nomenclature does not follow any official designation, two organizations (INHAND; https://www.toxpath.org/inhand.asp and National Cancer Institute Mouse Models of Cancer Consortium Tumor Pathology Nomenclature) have provided international nomenclatures for specific tissues [2, 14]. Other published guides are included in each appropriate organ chapter [15, 16]. Many books and refereed publications on mouse pathology provide valuable information for pathologists and scientists [12,17–35] as well as web sites (https://ntp.niehs.nih.gov/nnl; http://www.informatics.jax.org/frithbook; http://eulep.pdn.cam.ac.uk/~skinbase/index.php). Importantly, many of these references involve both DVMs and MDs, pathologists, and basic scientists, who integrate mouse and human disease nomenclature together to be state‐of‐the‐art. The pathology nomenclature used in this book generally reflects the NCI tumor pathology and INHAND general pathology nomenclatures. There are, however, no international or national standards for nomenclature that must be followed. These published nomenclatures are merely guidelines for use by scientists, pathologists, and journals. Each chapter author considered these guidelines and noted appropriate references for each organ and tissue.
Mouse Genetic Nomenclature
In contrast to pathology nomenclature, mouse genetic nomenclature is standardized. Chapter 3 focuses on the details of the nomenclature system and discusses how it was developed. While the authors and editors have, for the most part, updated the nomenclature, not all authors were willing to do so. Regardless, one can and should use the Mouse Genome Informatics website to verify all genes and alleles, as discussed in the Chapter 3, to make sure they are working with the correct nomenclature and allelic mutations.
Tumor Pathology
It is known in human and mouse pathology that cancer pathogenesis follows a scheme of molecular pathogenesis and an associated histopathogenesis [14, 16, 36]. There have been numerous publications on the role of specific genes in tumor pathogenesis in humans and animals. It is not the intention of this book to review the role of all genes for which published information on mouse cancer models is available, but rather to provide samples of some of the more common and important genes that play important roles. GEM may involve a single gene and attempt to mimic the human genetic disorder, or GEM may represent non‐familial genetic changes in the pathways to disease including cancer. Tumor frequency data in wild‐type control mice, especially in aging studies, have often been reported in various strains and stocks [1, 7, 23, 35, 37, 38]. While these reports provide general background information on the frequency of cancer types in a wildtype inbred strain, the actual frequency will vary based on substrain, husbandry, and other factors, necessitating the use of adequate numbers of control mice for studies on frequency of cancers in GEMs.
Immunohistochemistry (IHC), Scoring, Image Analysis, and Other Supportive Research Pathology Techniques
A variety of special pathology techniques are important adjuncts to mouse research. These include immunohistochemistry (IHC), in situ hybridization (ISH), ultrastructure, imaging, image analysis, artificial intelligence, machine learning, and a variety of molecular techniques. Most chapters will include examples of these for the various tissues. Some publications offer reviews of the use of IHC in mice [39–42] and Internet sites offer IHC protocols (http://tumor.informatics.jax.org/mtbwi/index.do, https://www.niehs.nih.gov/research/resources/protocols/protocols‐immuno/index.cfm) and whole slide images (http://tumor.informatics.jax.org/mtbwi/lymphomaPathology.jsp).
Histopathology scoring (grading) of lesion type and severity can often be used for mouse models of disease, genetics, and preclinical development for drugs [6, 34,43–45]. Examples are given in some chapters. The newer fields of image analysis, artificial intelligence, and machine learning СКАЧАТЬ